Comparative Analysis of the Aspergillus fumigatus Cell Wall Modification and Ensuing Human Dendritic Cell Responses by β-(1,3)-Glucan Synthase Inhibitors-Caspofungin and Enfumafungin.

IF 3.6 3区 生物学 Q2 MYCOLOGY Mycopathologia Pub Date : 2024-09-20 DOI:10.1007/s11046-024-00894-7
Karine Guilloux, Pushpa Hegde, Sarah Sze Wah Wong, Vishukumar Aimanianda, Jagadeesh Bayry, Jean-Paul Latgé
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Abstract

Caspofungin, a lipopeptide, is an antifungal drug that belong to the class of echinocandin. It inhibits fungal cell wall β-(1,3)-glucan synthase activity and is the second-line of drug for invasive aspergillosis, a fatal infection caused mainly by Aspergillus fumigatus. On the other hand, Enfumafungin is a natural triterpene glycoside also with a β-(1,3)-glucan synthase inhibitory activity and reported to have antifungal potential. In the present study, we compared the growth as well as modifications in the A. fumigatus cell wall upon treatment with Caspofungin or Enfumafungin, consequentially their immunomodulatory capacity on human dendritic cells. Caspofungin initially inhibited the growth of A. fumigatus, but the effect was lost over time. By contrast, Enfumafungin inhibited this fungal growth for the duration investigated. Both Caspofungin and Enfumafungin caused a decrease in the cell wall β-(1,3)-glucan content with a compensatory increase in the chitin, and to a minor extent they also affected cell wall galactose content. Treatment with these two antifungals did not result in the exposure of β-(1,3)-glucan on A. fumigatus mycelial surface. Enzymatic digestion suggested a modification of β-(1,3)-glucan structure, specifically its branching, upon Enfumafungin treatment. While there was no difference in the immunostimulatory capacity of antifungal treated A. fumigatus conidia, alkali soluble-fractions from Caspofungin treated mycelia weakly stimulated the dendritic cells, possibly due to an increased content of immunosuppressive polysaccharide galactosaminogalactan. Overall, we demonstrate a novel mechanism that Enfumafungin not only inhibits β-(1,3)-glucan synthase activity, but also causes modifications in the structure of β-(1,3)-glucan in the A. fumigatus cell wall.

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β-(1,3)-葡聚糖合成酶抑制剂--卡泊芬净和恩夫马芬净对曲霉菌细胞壁修饰和随之而来的人类树突状细胞反应的比较分析
卡泊芬净(Caspofungin)是一种脂肽类抗真菌药物,属于棘白菌素类。它能抑制真菌细胞壁β-(1,3)-葡聚糖合成酶的活性,是治疗侵袭性曲霉病的二线药物,侵袭性曲霉病主要是由烟曲霉引起的致命感染。另一方面,恩福菌素是一种天然三萜糖苷,也具有β-(1,3)-葡聚糖合成酶抑制活性,据报道具有抗真菌潜力。在本研究中,我们比较了用卡泊芬净或恩福芬净处理烟曲霉细胞壁后,烟曲霉细胞壁的生长和改变情况,以及它们对人类树突状细胞的免疫调节能力。卡泊芬净最初能抑制烟曲霉的生长,但随着时间的推移,效果逐渐消失。与此相反,恩福明在调查的持续时间内都能抑制这种真菌的生长。卡泊芬净和恩福芬净都会导致细胞壁中的β-(1,3)-葡聚糖含量下降,而几丁质含量则会相应增加。用这两种抗真菌剂处理不会导致烟曲霉菌丝体表面的β-(1,3)-葡聚糖暴露。酶解结果表明,恩福菌素处理后,β-(1,3)-葡聚糖结构发生了改变,特别是其分支。虽然经抗真菌处理的烟曲霉分生孢子的免疫刺激能力没有差异,但经Caspofungin处理的菌丝体的碱溶性馏分对树突状细胞的刺激作用较弱,这可能是由于免疫抑制性多糖半乳糖氨基半乳聚糖的含量增加所致。总之,我们证明了一种新的机制,即恩福明不仅能抑制β-(1,3)-葡聚糖合成酶的活性,还能改变烟曲霉细胞壁中β-(1,3)-葡聚糖的结构。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Mycopathologia
Mycopathologia 生物-真菌学
CiteScore
6.80
自引率
3.60%
发文量
76
审稿时长
3 months
期刊介绍: Mycopathologia is an official journal of the International Union of Microbiological Societies (IUMS). Mycopathologia was founded in 1938 with the mission to ‘diffuse the understanding of fungal diseases in man and animals among mycologists’. Many of the milestones discoveries in the field of medical mycology have been communicated through the pages of this journal. Mycopathologia covers a diverse, interdisciplinary range of topics that is unique in breadth and depth. The journal publishes peer-reviewed, original articles highlighting important developments concerning medically important fungi and fungal diseases. The journal highlights important developments in fungal systematics and taxonomy, laboratory diagnosis of fungal infections, antifungal drugs, clinical presentation and treatment, and epidemiology of fungal diseases globally. Timely opinion articles, mini-reviews, and other communications are usually invited at the discretion of the editorial board. Unique case reports highlighting unprecedented progress in the diagnosis and treatment of fungal infections, are published in every issue of the journal. MycopathologiaIMAGE is another regular feature for a brief clinical report of potential interest to a mixed audience of physicians and laboratory scientists. MycopathologiaGENOME is designed for the rapid publication of new genomes of human and animal pathogenic fungi using a checklist-based, standardized format.
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